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Fabrication and functionalization of single asymmetric nanochannels for electrostatic/hydrophobic association of protein molecules

机译:蛋白质分子的静电/疏水缔合的单个不对称纳米通道的制备和功能化

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摘要

We have developed a facile and reproducible method for surfactant-controlled track-etching and chemical functionalization of single asymmetric nanochannels in PET (polyethylene terephthalate) membranes. Carboxyl groups present on the channel surface were converted into pentafluorophenyl esters using EDC/PFP (N-(3-dimethylaminopropyl)-N'-ethylcarbodiimide hydrochloride/pentafluorophenol) coupling chemistry. The resulting amine-reactive esters were further covalently coupled with ethylenediamine or propylamine in order to manipulate the charge polarity and hydrophilicity of the nanochannels, respectively. Characterization of the modified channels was done by measuring their current-voltage (I-V) curves as well as their permselectivity before and after the chemical modification. The electrostatic/hydrophobic association of bovine serum albumin on the channel surface was observed through the change in rectification behaviour upon the variation of pH values.
机译:我们已经开发了一种简便且可重现的方法,用于在PET(聚对苯二甲酸乙二醇酯)膜中对单个不对称纳米通道进行表面活性剂控制的轨迹蚀刻和化学功能化。使用EDC / PFP(N-(3-二甲基氨基丙基)-N'-乙基碳二亚胺盐酸盐/五氟苯酚)偶联化学方法,将通道表面上存在的羧基转化为五氟苯基酯。将所得的胺反应性酯进一步与乙二胺或丙胺共价偶联,以分别控制纳米通道的电荷极性和亲水性。通过测量化学修饰前后的电流-电压(I-V)曲线及其通透性,可以对修饰通道进行表征。通过pH值变化时整流行为的变化,可以观察到牛血清白蛋白在通道表面上的静电/疏水缔合。

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